A drug carrier able to reach the brain, bind to an aggressive type of tumor called glioblastoma multiforme, and release a chemotherapeutic agent has been tested for the first time by Brazilian researchers. According to an article published in the International Journal of Pharmaceutics, the potential treatment was shown to be effective in isolated cells and animal models thanks to a combination of nanotechnology, chemotherapy and a monoclonal antibody.
Glioblastoma multiforme accounts for 60% of all brain tumors in adults and is also the most aggressive type of brain cancer. Even after surgery, radiation therapy and conventional chemotherapy, patient survival averages about 14 months. One of the reasons is angiogenesis, a process whereby the tumor quickly creates its own blood vessels in order to develop.
“Another difficulty is the blood-brain barrier, which prevents drugs from reaching the tumor,” said Leonardo Di Filippo, a doctoral candidate and researcher at São Paulo State University’s School of Pharmaceutical Sciences in Araraquara (FCFAr-UNESP).
To address these challenges, Di Filippo worked with fellow researchers at UNESP and two other Brazilian institutions, the University of Campinas (UNICAMP) and the University of São Paulo (USP) at Ribeirão Preto, to combine docetaxel, a powerful chemotherapy drug, with a nanostructured lipid carrier designed to cross the blood-brain barrier. “We developed a formulation in which the substances were combined in a stable manner,” he said.
The researchers also coupled the carrier to bevacizumab, a monoclonal antibody developed against vascular endothelial growth factor (VEGF) and approved for other uses. “VEGF is the cancer protein that stimulates angiogenesis and tends to be overexpressed in glioblastoma multiforme,” Di Filippo explained. The goal was to create a formulation capable of penetrating the brain and releasing a chemotherapy drug to destroy the tumor.
Having created the nanostructured lipid carrier with docetaxel and bevacizumab, the researchers set out to make sure it met certain basic criteria. Laboratory tests showed its size to be 128 nanometers, small enough to overcome the blood-brain barrier. In addition, docetaxel entrapment was 90% and bevacizumab coupling efficiency was 62%. “Those are positive numbers, sufficient to guarantee adequate therapeutic concentrations,” Di Filippo said.
The next step was an assessment of the compound’s effects on two glioblastoma cell lines and healthy cells. The nanocarrier eliminated five times more cancer cells than docetaxel on its own without affecting healthy cells. It was particularly effective against U87MG, a glioblastoma cell that overexpresses VEGF, but less so against A172, which expresses relatively little VEGF. “These findings show that our nanocarrier selectively attacks cells that express a lot of VEGF,” Di Filippo said.
The researchers also found that the potential medication was able to enter cancer cells and release docetaxel continuously for about 84 hours, suggesting prolonged availability of the chemotherapy drug in the organism.
Good results in animals
Using techniques developed by the UNICAMP team, rats were inoculated with glioma cells (glioma is a type of cancer similar to glioblastoma). Five days later they were divided into six groups: treatment with placebo; docetaxel alone; nanocarrier alone, without bevacizumab or docetaxel; nanocarrier and bevacizumab, without docetaxel; nanocarrier and docetaxel, without bevacizumab; nanocarrier with docetaxel and bevacizumab.
After 15 days, the first four groups were found not to have benefited from the treatment. In the fifth group (nanocarrier with docetaxel) and sixth group (nanocarrier with docetaxel and bevacizumab), tumor volume was reduced by 40% and 70% respectively. “These are significant numbers for trials of this kind,” Chorilli said.
The researchers also found that the formulation did not cause any deterioration in levels of biomarkers such as albumin and creatinine compared with the use of docetaxel on its own. “This shows that toxicity was not intensified,” Di Filippo explained.
According to Chorilli, the results were positive but these were the first experiments with the nanostructured lipid carrier for this specific application. “We need to conduct more studies using isolated cells and animals. If the results against glioblastoma multiforme remain good, we could try to find partners for clinical trials with human volunteers,” he said.
The study reported in the article highlighted the potential of lipid nanocarriers in treating brain cancer, he added: “We can use different combinations with other monoclonal antibodies and chemotherapy drugs against other types of cancer. Many more years will undoubtedly be required to complete this research.”
Chorilli is studying similar methods for the treatment of infections, such as gastritis and other diseases caused by the bacterium Helicobacter pylori, in research also supported by FAPESP.
About São Paulo Research Foundation (FAPESP)
The São Paulo Research Foundation (FAPESP) is a public institution with the mission of supporting scientific research in all fields of knowledge by awarding scholarships, fellowships and grants to investigators linked with higher education and research institutions in the State of São Paulo, Brazil. FAPESP is aware that the very best research can only be done by working with the best researchers internationally. Therefore, it has established partnerships with funding agencies, higher education, private companies, and research organizations in other countries known for the quality of their research and has been encouraging scientists funded by its grants to further develop their international collaboration. You can learn more about FAPESP at www.fapesp.br/en and visit FAPESP news agency at www.agencia.fapesp.br/en to keep updated with the latest scientific breakthroughs FAPESP helps achieve through its many programs, awards and research centers. You may also subscribe to FAPESP news agency at http://agencia.fapesp.br/subscribe.
International Journal of Pharmaceutics
Glioblastoma multiforme targeted delivery of docetaxel using bevacizumab-modified nanostructured lipid carriers impair in vitro cell growth and in vivo tumor progression
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